104329-18-2

Basic information

• Product Name: 4-chloro-N-[(4-methoxyphenyl)methyl]aniline
• Synonyms: 4-chloro-N-[(4-methoxyphenyl)methyl]aniline;(4-CHLOROPHENYL)(4-METHOXYBENZYL)AMINE;OTAVA-BB 1397132;4-Chloro-N-(4-Methoxybenzyl)aniline, 97%;N-(4-CHLOROPHENYL)-4-METHOXYBENZYLAMINE
• CAS NO: 104329-18-2
• Molecular Formula: C₁₄H₁₄ClNO
• Molecular Weight: 247.724
• Mol File: 104329-18-2.mol
• Article Data: 33

Chemical Properties

• Appearance: /
• CAS DataBase Reference: 4-chloro-N-[(4-methoxyphenyl)methyl]aniline(CAS DataBase Reference)
• NIST Chemistry Reference: 4-chloro-N-[(4-methoxyphenyl)methyl]aniline(104329-18-2)
• EPA Substance Registry System: 4-chloro-N-[(4-methoxyphenyl)methyl]aniline(104329-18-2)

Safety Data

• Hazardous Substances Data: 104329-18-2(Hazardous Substances Data)

Upstream product

• 15485-22-0 4-chloro-N-[(4-methoxyphenyl)methylidene]aniline 
• 599-89-3 4-chlorophenyl p-toluenesulfonate 
• 2393-23-9 4-methoxy-benzylamine 
• 80-38-6 fenson 
• 80-33-1 chlorofensone 
• 128886-84-0 p-Chlorophenyl p-nitrobenzenesulphonate 
• 106-47-8 4-chloro-aniline 
• 123-11-5 4-methoxy-benzaldehyde 
• 104-88-1 4-chlorobenzaldehyde 
• 104-94-9 4-methoxy-aniline 
• 824-94-2 p-methoxybenzyl chloride 
• 98986-86-8 (E)-N-(4-chlorophenyl)-1-(4-methoxyphenyl)methanimine 
• 100-00-5 4-chlorobenzonitrile 
• 637-87-6 1-Chloro-4-iodobenzene 

Downstream Products

• 1621686-49-4 5-chloro-3-[hydroxy(thiophen-2-yl)methylene]-1-(4-methoxybenzyl)indolin-2-one 
• 1621686-44-9 N-(4-chlorophenyl)-2-diazo-N-(4-methoxybenzyl)-3-oxo-3-(thiophen-2-yl)propanamide 
• 15485-22-0 4-chloro-N-[(4-methoxyphenyl)methylidene]aniline 
• 936840-10-7 CH₂OC₁₅H₁₂NCl 

Relevant articles and documents

Highly active, low-valence molybdenum- and tungsten-amide catalysts for bifunctional imine-hydrogenation reactions

The reactions of [M(NO)(CO)4(ClAlCl3)] (M=Mo, W) with (iPr2PCH2CH2)2NH, (PNHP) at 90 °C afforded [M(NO)(CO)(PNHP)Cl] complexes (M=Mo, 1 a; W, 1 b). The treatment of co

Designed pincer ligand supported Co(ii)-based catalysts for dehydrogenative activation of alcohols: Studies onN-alkylation of amines, α-alkylation of ketones and synthesis of quinolines

Base-metal catalystsCo1,Co2andCo3were synthesized from designed pincer ligandsL1,L2andL3having NNN donor atoms respectively.Co1,Co2andCo3were characterized by IR, UV-Vis. and ESI-MS spectroscopic studies. Single crystal X-ray diffraction studies were investigated to authenticate the molecular structures ofCo1andCo3. CatalystsCo1,Co2andCo3were utilized to study the dehydrogenative activation of alcohols forN-alkylation of amines, α-alkylation of ketones and synthesis of quinolines. Under optimized reaction conditions, a broad range of substrates including alcohols, anilines and ketones were exploited. A series of control experiments forN-alkylation of amines, α-alkylation of ketones and synthesis of quinolines were examined to understand the reaction pathway. ESI-MS spectral studies were investigated to characterize cobalt-alkoxide and cobalt-hydride intermediates. Reduction of styrene by evolved hydrogen gas during the reaction was investigated to authenticate the dehydrogenative nature of the catalysts. Probable reaction pathways were proposed forN-alkylation of amines, α-alkylation of ketones and synthesis of quinolines on the basis of control experiments and detection of reaction intermediates.

Design, synthesis and evaluation of novel bis-substituted aromatic amide dithiocarbamate derivatives as colchicine site tubulin polymerization inhibitors with potent anticancer activities

As the continuation of our work on the development of tubulin inhibitors with potential anticancer activities, novel bis-substituted aromatic amide dithiocarbamate derivatives were designed by contacting bis-substituted aryl scaffolds (potential anti-tubulin fragments) with N-containing heterocycles (potential anti-tubulin fragments) in one hybrid using the anticancer dithioformate unit as the linker. The antiproliferative activity against three digestive tract tumor cells was evaluated and preliminary structure activity relationships were summarized. Among these compounds, compound 20q exhibited most potent antiproliferative activity against MGC-803, HCT-116, Kyse30 and Kyse450 cells with IC50 values of 0.084, 0.227, 0.069 and 0.078 μM, respectively. In further studies, compound 20q was identified as a novel tubulin inhibitor targeting the colchicine binding site. Compound 20q could inhibit the microtubule assembly and disrupt cytoskeleton in Kyse30 and Kyse450 cells. The results of molecular docking suggested that compound 20q could tightly bind into the colchicine binding site of tubulin by hydrogen bonds and hydrophobic interactions. Compound 20q dose-dependently inhibited the cell growth and colony formation, effectively arrested cells at the G2/M phase and induce mitochondrial apoptosis in Kyse30 and Kyse450 cells. In addition, Compound 20q could regulate the expression of G2/M phase and mitochondrial apoptosis related proteins. Collectively, compound 20q was here reported as a novel tubulin inhibitor with potential anticancer activities.

Switchable Imine and Amine Synthesis Catalyzed by a Well-Defined Cobalt Complex

Switchable imine and amine synthesis catalyzed by a tripodal ligand-supported well-defined cobalt complex is presented herein. A large variety of primary alcohols and amines were selectively converted to imines or amines in good to excellent yields. It is discovered that the base plays a crucial role on the selectivity. A catalytic amount of base leads to the imine formation, while an excess loading of base results in the amine product. This strategy on product selectivity also strongly depends on the organometallic catalysts in use. We expect that the present study could provide useful insights toward selective organic synthesis and catalyst design.